Comparative Toxicokinetics of Bisphenol S in Rats and Mice Following Gavage Administration

Overview

Journal Toxicol Appl Pharmacol

Specialties Pharmacology
Toxicology

Date 2020 Aug 28

PMID 32853628

Citations 2

Authors

Suramya Waidyanatha

Sherry R Black

Melanie Silinski

Vicki Sutherland

Brenda L Fletcher

Reshan A Fernando

Timothy R Fennell

Affiliations

Soon will be listed here.

Abstract

Bisphenol S (BPS) is a component of polyether sulfone used in a variety of industrial applications and consumer products. We investigated the plasma toxicokinetic (TK) behavior of free (unconjugated parent) and total (parent and conjugated) BPS in rats and mice following a single gavage administration (34, 110, or 340 mg/kg). In male rats, BPS was rapidly absorbed with free BPS maximum concentration (C) reached at ≤2.27 h. Elimination of free BPS in male rats was dose-dependent with estimated half-lives of 5.77-11.9 h. C and area under the concentration versus time curve (AUC) increased with dose although the increase in AUC was more than dose proportional. In male rats, total BPS C was reached ≤2.77 h with both C (≥ 10-fold) and AUC (≥ 15-fold) higher than free BPS demonstrating rapid and extensive conjugation of BPS. In male mice, the increase in C and AUC of free BPS was dose-proportional; C was higher and AUC was lower than in male rats. BPS was cleared more rapidly in male mice (half-life 2.86-4.21 h) compared to male rats (half-life 5.77-11.9 h). Similar to rats, total BPS C (≥ 6-fold) and AUC (≥ 12-fold) were higher than corresponding free BPS. Oral bioavailability of free BPS was low to moderate (rats, ≤ 21%; mice, ≤ 19%). There were some species differences in TK parameters of free and total BPS and limited sex difference in rats and mice. In addition, there were dose-related effects of plasma TK parameters in rats.

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